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Bivalent Vaccine Effectiveness Against Type-Specific HPV Positivity: Evidence for Cross-Protection Against Oncogenic Types among Dutch STI Clinic Visitors

  • D. Adema
  • , R. Buist-Arkema
  • , A. Beerens
  • , D. Luijt
  • , S. Meijer
  • , J. Schirm
  • , M. Peeters
  • , J. Rossen
  • , H. Verbakel
  • , P. Van Esch
  • , J. Verweij
  • , A. Van Der Eijk
  • , R. Huisman
  • , C. Kerkhof
  • , H. Korff
  • , M. Schutten
  • , J. Velzing
  • , F. Verduyn-Lunel
  • , S. Lakbiach
  • , P. Van Rosmalen
  • R. Schuurman, D. Abma, K. Adams, S. Bruisten, I. Linde, P. Oostvogel, C. Touwen, W. Vermeulen, A. Brink, J. Nelissen, P. Wolffs, N. Duijvendijk, P. Schneeberger, M. D. Innissen Van Poppel, W. Melchers, Y. Poort, M. Hooghiemstra, H. Huisman, J. Weel, F. Bosma, F. Geeraedts, I. Polman, P. van Goor, M. Wolfhagen, C. de Mooij, E. Van Koolwijk, M. Peters, C. Swanink, R. Tiemessen, T. Van Zwet, J. Janssen, M. Pelsers, W. de Waal, G. Aalfs, J. Kiewiet, P. Sanders, H. Van Buel-Bruins, C. Van Bokhoven-Rombouts, P. Cornelissen, M. Kersten, C. Van Ruitenbeek, I. Molenaar, E. Doorn, L. Masthoff, E. Pannekoek, V. Sigurdsson, M. Bugter, H. Götz, M. Illidge-Onder de Linden, M. Mattijssen, J. Stam, E. Swaders, F. De Groot, F. Postma, E. Brouwers, A. Niekamp, M. Smit, A. Botraby, D. Bukasa, C. De Haan, P. Hut-van Vliet, T. Taconis, M. De Graas, I. Hondelink, C. Kampman, A. Gelissen-Hansen, I. De Koning, H. Van Kruchten, M. Van De Pas, H. Fennema, T. Heijman, A. Hogewoning, A. Van Leeuwen, M. Van Rooijen, F. Neienhuijsen, M. Pelgrim, Medical Microbiological Laboratories, and the Public Health Services

Research output: Contribution to journalArticleAcademicpeer-review

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Abstract

Background. Observational postmarketing studies are important to assess vaccine effectiveness (VE). We estimated VE from the bivalent human papillomavirus (HPV) vaccine against HPV positivity of vaccine and nonvaccine types in a high-risk population. Methods. We included all vaccine-eligible women from the PASSYON study, a biennial cross-sectional survey in Dutch sexually transmitted infection clinics. Vaginal swabs were analyzed using a polymerase chain reaction-based assay (SPF10-LiPA25) able to detect the 12 high-risk HPV (hrHPV) types 16/18/31/33/35/39/45/51/52/56/58/59. We compared hrHPV positivity between self-reported vaccinated (.1 dose) and unvaccinated women, and estimated VE by a logistic mixed model. Results. We included 1087 women of which 53% were hrHPV positive and 60% reported to be vaccinated. The adjusted pooled VE against HPV-16/18 was 89.9% (81.7%.94.4%). Moreover, we calculated significant VE against nonvaccine types HPV-45 (91%), HPV-35 (57%), HPV-31 (50%), and HPV-52 (37%). Among women who were offered vaccination 5/6 years ago, we estimated similar VE against HPV-16/18 (92%) and all hrHPV types (35%) compared to women who were offered vaccination <5 years ago (83% and 33%, respectively). Conclusion. We demonstrated high VE of the bivalent vaccine against HPV-16/18 and cross-protection against HPV-45/35/31/52. Protection against HPV-16/18 was sustained up to 6 years postvaccination.
Original languageEnglish
Pages (from-to)213-222
Number of pages10
JournalJournal of infectious diseases
Volume217
Issue number2
Early online date11 Nov 2017
DOIs
Publication statusPublished - 15 Jan 2018

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

  1. SDG 3 - Good Health and Well-being
    SDG 3 Good Health and Well-being

Keywords

  • Journal Article

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